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Fluorescent Kinase Probes Enabling Identification and Dynamic Imaging of HER2(+) Cells

机译:荧光激酶探针能够鉴定和动态成像HER2(+)细胞。

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The human epidermal growth factor receptor, EGFR/ERBB/HER, family of receptor tyrosine kinases is central to many signaling pathways and a validated chemotherapy target in multiple cancers. While EGFR/ERBB-targeted therapies, including monoclonal antibodies, e.g., trastuzumab, and small molecule kinase inhibitors, such as lapatinib, have been developed, rapid identification and classification of cancer cells is key to identifying the best treatment regime. We report ERBB2 (also HER2) targeting kinase probes that exhibit a "turn-on" emission response upon binding. These live cell compatible probes differentiate ERBB2(+) cells from low-level, ERBB2() cells by targeting the intracellular ATP-binding pocket of ERBB2 with therapeutic inhibitor-like specificity. Beyond kinase expression levels, probe signal is linked to the phosphotyrosine-correlated activation state of the ERBB2 population. Additionally, the rapid signaling capability of the probes can report changes in activation state in live cells providing a unique type of complementary information to immunohistochemical assays of receptor kinase populations.
机译:人表皮生长因子受体EGFR / ERBB / HER酪氨酸激酶家族是许多信号通路的核心,也是多种癌症中有效的化疗靶标。虽然已经开发出靶向EGFR / ERBB的疗法,包括单克隆抗体(例如曲妥珠单抗)和小分子激酶抑制剂(例如拉帕替尼),但癌细胞的快速鉴定和分类是鉴定最佳治疗方案的关键。我们报告了ERBB2(也有HER2)靶向激酶探针结合后显示“打开”发射响应。这些活细胞兼容探针通过以治疗性抑制剂样特异性靶向ERBB2的胞内ATP结合口袋,将ERBB2(+)细胞与低水平的ERBB2()细胞区分开。除激酶表达水平外,探针信号还与ERBB2群体的磷酸酪氨酸相关的激活状态有关。另外,探针的快速信号传导能力可以报告活细胞中激活状态的变化,从而为受体激酶群体的免疫组织化学分析提供独特类型的补充信息。

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